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1. Cyprocide selectively kills nematodes via cytochrome P450 bioactivation

2. Molecular evidence of widespread benzimidazole drug resistance in Ancylostoma caninum from domestic dogs throughout the USA and discovery of a novel β-tubulin benzimidazole resistance mutation

5. Species richness, distribution and genetic diversity of Caenorhabditis nematodes in a remote tropical rainforest

9. C. elegans as a model for inter-individual variation in metabolism

11. Shared Genomic Regions Underlie Natural Variation in Diverse Toxin Responses

17. Quantitative tests of albendazole resistance in beta-tubulin mutants

18. Quantifying the fitness effects of resistance alleles with and without anthelmintic selection pressure usingCaenorhabditis elegans

24. Glial expression of a steroidogenic enzyme underlies natural variation in hitchhiking behavior.

25. Quantifying the fitness effects of resistance alleles with and without anthelmintic selection pressure using Caenorhabditis elegans.

26. The Genetic Basis of Natural Variation in Caenorhabditis elegans Telomere Length

27. Remarkably Divergent Regions Punctuate the Genome Assembly of the Caenorhabditis elegans Hawaiian Strain CB4856

28. A Powerful New Quantitative Genetics Platform, Combining Caenorhabditis elegans High-Throughput Fitness Assays with a Large Collection of Recombinant Strains

29. A variant in the neuropeptide receptor npr-1 is a major determinant of Caenorhabditis elegans growth and physiology.

30. Diverse Plant-Parasitic Nematodes are Selectively Killed by Oxadiazole Thioether Pro-Nematicides

34. Chromosome-scale selective sweeps shape Caenorhabditis elegans genomic diversity

35. Natural genetic variation in the pheromone production of C. elegans

39. CaeNDR, the Caenorhabditis Natural Diversity Resource.

40. Chapter Three - Getting around the roundworms: Identifying knowledge gaps and research priorities for the ascarids.

47. Natural genetic variation in the pheromone production ofC. elegans

48. An anchored experimental design and meta-analysis approach to address batch effects in large-scale metabolomics

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